Differentiation of porcine T helper cells is still poorly investigated, partly due to a lack of monoclonal antibodies (mAbs) specific for molecules involved in this process. Recently, we identified a mAb specific for porcine CD27 and showed that CD27 is expressed by all naïve CD8a+ T helper cells but divides CD8a- T helper cells into a CD27+ and a CD27- subset. In the present study, detailed phenotypical and functional analyses of these T-helper cell subpopulations were performed. Naïve CD8a+CD27+ T helper cells predominantly resided in various lymph nodes, whereas higher proportions of CD8a-CD27 + and CD8a-CD27- T helper cells were found in blood, spleen and liver. Both CD8a-CD27+ and CD8a -CD27- T helper cells were capable of producing IFN-γ upon in vitro polyclonal stimulation and antigen-specific restimulation. Experiments with sorted CD8a+CD27+, CD8a-CD27+ and CD8a-CD27- T-helper cell subsets following polyclonal stimulation revealed the lowest proliferative response but the highest ability for IFN-γ and TNF- production in the CD8a-CD27- subset. Therefore, these cells resembled terminally differentiated effector memory cells as described in human. This was supported by analyses of CCR7 and CD62L expression. CD8a-CD27 - T helper cells were mostly CCR7- and had considerably reduced CD62L mRNA levels. In contrast, expression of both homing-receptors was increased on CD8a-CD27+ T helper cells, which also had a proliferation rate similar to naïve CD8a+CD27+ T helper cells and showed intermediate levels of cytokine production. Therefore, similar to human, CD8a-CD27+ T helper cells displayed a phenotype and functional properties of central memory cells. © 2013 Reutner et al.; licensee BioMed Central Ltd.
CITATION STYLE
Reutner, K., Leitner, J., Müllebner, A., Ladinig, A., Essler, S. E., Duvigneau, J. C., … Gerner, W. (2013). CD27 expression discriminates porcine T helper cells with functionally distinct properties. Veterinary Research, 44(1). https://doi.org/10.1186/1297-9716-44-18
Mendeley helps you to discover research relevant for your work.